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Organotin Alkoxides and Amines: New Chemistry and Applications JEAN-CLAUDE POMMIER and MICHEL PEREYRE Laboratoire de Chimie Organique, Laboratoire des Composés Organiques et de l'Etain, associé au C.N.R.S., Université de Bordeaux I, 33405-Talence, France
du
Silicium
This paper deals with some aspects of organotin alkoxide and amine chemistry, mainly centered on the work done in Bordeaux. The first part includes some new preparations of organotin alkoxides and some of their properties: exchange reactions in organometallic chemistry, nucleophilic substitution either internal (with halides or oxiranes) or intermolecular (αhaloketones, alkylation of enolates), and finally oxidation to carbonyl derivatives. The behavior of organotin amines in nu cleophilic displacement of α-haloketones and organic dihalides is investigated. They undergo either substitution or ad dition with carbonyl derivatives, depending on electronic and steric factors. An extension of these reactions to organotin enolates affords a route to organic enamines or, more inter estingly, to organotin enamines. Some new preparations of this last class of compounds are reported.
T
his review discusses some aspects of organotin (alkoxide and amine) chemistry mainly centered on the work of the Bordeaux group during the past five years and does not claim to be complete, the references cited being only examples. In particular, work done before 1970 has been omitted since it was been the subject of other papers or books (I, 2, 3, 4, 5, 6, 7). Introduction Organotin derivatives of alcohol and amines exhibit special properties owing to two conflicting factors: (1) Formally they are metal alkoxides or amides, the nucleophilic character of the oxygen or nitrogen being enhanced, as in the corresponding compounds derived from Group I or II metals. (2) The electropositive nature of tin is quite low among metals, and, con sequently, bonds involving oxygen or nitrogen are rather covalent and exhibit 82
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
6.
POMMIER
Alkoxides and Amines
A N D PEREYRE
83
special reactivity. They are covalent in physical properties, they are generally liquids or low melting solids, and they may often react neat. The reactions reported here relate to both these properties. A striking and general observation is that although they behave like their more electropositive analogues, they are less reactive and, therefore, often much more selective.
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Organotin Alkoxides Preparations. Depending on the final use of alkoxide, different methods of preparation may be used. To take advantage of the alkoxide properties (which is generally the case), the best and easiest route is that described by Da vies et al., (8, 9, 10, 11) involving a fast and rapid reaction between the commercially available organotin oxides and alkyl carbonates. R SnO
+
C C W — • 2R SnOR'
+ C0
2
RzSnO
+
COaR/
+ C0
2
6
3
—
R^niOR'^
From these tin alkoxides, other compounds containing tin-oxygen bonds can be prepared using a transalkoxylation or a transesterif ication procedure (see, for example, Refs. 12,13,15,16,17,18,19, 21, 22, 23): =SnOR' =SnOR'
+ +
ROH — • =SnOR AcOR
—
+ R'OH
=SnOR
+
AcOR'
In the past few years, other methods have been reported but mainly with interest in the organotin compound itself: (1) the metathesis between a metal alkoxide and an organotin halide (24,25,26), (2) reaction between tin oxides and alcohols (10,27,28) (particularly efficient for high boiling alcohols), and (3) alcoholysis of organotin amides (14, 20, 29, 30, 31). Other miscellaneous methods have been reported in special cases using an interfacial technique (32), disproportionation (33,34), the ring opening of oxiranes (35, 36), and reactions of magnesium alcoholates with dialkyltin oxides (37). A new and very convenient method was found here (38) for preparing trimethyland dimethylphenyltin alkoxides based on an exchange between the easily available tributyltin alkoxides and the corresponding organotin bromides. For example: BuaSnOR
+
Me SnBr 3
—•
Me SnOR 3
+
Bu SnBr 3
( R = M e 7 5 % ; E t :80%) Bu SnOMe 3
+
0Me SnBr — • 2
Me SnOMe 2
+
B u S n B r (80%) 3
It seems probable that the more efficient coordinating ability of the final organotin alkoxide provides the driving force for this type of reaction. Although tributylin methoxide is involved in the exchange of the methoxide groups observed by N M R
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
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84
ORGANOTIN COMPOUNDS: NEW
CHEMISTRY A N D APPLICATIONS
(10,39), no evidence of coordination appears in its IR (41 ), whereas a strong association was found in the case of the trimethyltin analogue (40). This brief overview of the different preparations of organotin alkoxides shows that such compounds are easily prepared either to study their own chemistry or for synthetic purposes. Exchange Reactions: Use in Organometallic Chemistry. According to the Pearson theory, tin is a softer acid than silicon or germanium and thus links preferentially to soft bases. Accordingly, many exchanges involving the final formation of a silicon or germanium-oxygen bonds have been reported such as with M - X (X = halogen), M - S , M - N , or even M - H (M = Si or Ge). Since our initial discovery (42) of the exchange between tin alkoxides and chlorosilanes, =
SnOR
+
ssSiCl
—
==SnCl
+
=SiOR
many applications of this reaction have been applied to the preparation of a variety of organosilicon or germanium derivatives (43-55). Many of these reports deal with the preparations of organosilicon or germanium enolates from the corresponding organotin derivative. A n extension of these reactions to other heteroelements like sulfur (49,56,57) or nitrogen (58) may also be found in the literature. During the past five years, our interest in this aspect of organometallic chemistry has been concentrated on the mechanism of the exchange between silanes and organotin alkoxides, a basic reaction for the preparation of organotin hydrides (44, 59, 60, 61, 62). R SnOR' + 3
R" SiH — •
RgSnH +
3
R" SiOR' 3
Optically active organosilicon hydrides were used to study isotopic and substituent effects on the rate of reaction. The results (63, 64, 65) show a net retention of configuration at the silicon center, a positive primary kinetic isotopic effect, and a high activation entropy. Furthermore, the rate enhancement by either electron withdrawing groups on the silane or electron releasing groups on the organotin compound is in accordance with a rate determining step in which R
= S n — - 0 I
ssSi—H
4-
=Sn—OR
=Sn—Ô—R
I=sSi—H
= S n — H
+
=Si—OR
2
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
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6.
POMMIER
A N D
PEREYRE
Alkoxides and Amines
85
the incipient O - S i bond is more developed than the S n - H bond. These facts agree with either an Sni-Si mechanism (1) or with a two-step mechanism via an unstable pentacoordinated silicon intermediate occuring between two transition states of comparable energy (2). Nucleophilic Substitution at a Carbon Center. Organotin alkoxides act as nucleophiles toward organic and organometallic halides. However, with alkyl halides their reactivity is quite low (66) since good yields are only obtained with the more reactive halides (allylic or benzylic derivatives). However, in some cases this reaction is synthetically useful such as with chloromethylethers (55), tosyl chloride (23) sulfamoyl chloride (96), acid chlorides (69, 70, 67), cyanogen chloride (71), thyonyl chloride (72), phosgene (73), etc. Intramolecular Nucleophilic Substitution Organotin Halogenoalkoxides. The general scheme of this reaction is an intramolecular substitution leading to an oxygenated heterocycle:
R Sn—Ο 3
X
—
R SnX +
cT)
3
The starting organotin alkoxide can be readily obtained from tributyltin methoxide and the corresponding halohydrin:
R SnOMe }
+
HO
X
—•
X
RgSn—Ο
+
MeOH
These alkoxides are generally thermally unstable and decompose at various temperatures depending on ring size of the product heterocycle, the nature of the halogen, the substitution of the carbon bearing the oxygen and, in some cases, the configuration of the molecule (74). For oxiranes (75), some interesting features have been observed: the re action is completely a stereospecific process: BujjSnBr Me—CH—CH—Me J J Bu SnO Br erythro 3
meso
Me—CH—CH—Me 30min
f
\^ 0
trans-90% ( + 1 0 % of ketone, see below) cis-90% ( + 1 0 % of ketone* see below)
The necessity of this condition is demonstrated by the following examples taken from the cyclohexyl series (76):
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
86
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND APPLICATIONS Br
Bu SnBr 3
I
82%
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SnBu
;J
Br 0 Η
150 °C
•OSnBu , :
+
30min
Bu SnBr 3
77%
Η
The former reaction proceeds via a nucleophilic intramolecular displacement by the oxygen:
sSn—or The latter by a hydride migration: ^Br
When the antiposition is substituted as in the example shown below, a transposition occurs leading to a reduction in ring size.
0—Sn= Me
—
Q ^ - C — M e 0
+
(~y=0
C
+
Bu SnX 3
Me
X = C1:40% X = Br:80%
The hydride migration is a much more energetic process than the formation of oxiranes, and thus the decomposition of the halogenalkoxides at high tern-
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
6.
Alkoxides and Amines
POMMIER A N D PEREYRE
87
peratures leads to a mixture of oxiranes and ketones while formation of the latter can be avoided by using milder conditions:
ι ς η
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Me—CH—CH
Γ
/
30min
χ
i20»
Me—CH—CH Br
I
.
Me—C—Me
2
Ο
0
2
Bu,SnO
Me—CH—CH
C>
3hr
\
2
/
100%
Obviously, the latter conditions are more favorable for synthetic purposes. The study of this type of compound also shows clearly the influence of the substitution of the carbon bearing the oxygen; the more extensive the substitution, the easier the decomposition of the corresponding alkoxide. For example, for total reaction in 30 min, the organotin derivative of l-bromo-2-propanol needs to be heated to 150 °C, whereas the derivative of l-bromo-2-methyl-2-propanol is decomposed at temperatures as low as 70 °C. This fact parallels the nucleo philic character of the oxygen and corresponds to the situation observed in all the cases which have been studied. A further important factor on the relative ease of the reactions is the nature of the halogen. Two striking examples taken in the cyclohexyl series are given below:
a a
„OSnBu OSnBu
S
3
C1
91%
Buu; ^O OS S nn B
3
^Br
82%
Considering these observations, the hydride migration and the effect of the halogen on the rate of the reaction, it is expected that side reactions will occur more readily with the chlorine derivatives. Thus, for synthetic purposes, it is better to start with a bromoalkoxide. The case of the 3-haloalkoxide is of particular interest since it provides a very useful and sometimes unique route to oxetanes (77, 78):
I
I
I
= S n — O — C — C — C — X
III
r—Ί
—
=SnX
+
·
J
0
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
88
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND APPLICATIONS
The following examples are typical ,—ν
^O OS n B u ,
\_J\
CH,CH,Br
Bu3SnOCH>C H,CHCH Br
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()
2
,—ν
„
W
30min 200 C
30 mi η
*
_
C«H,-<
V / \
Ν/
0
+
C H,CH=CH . ( i
2
Λ
90%
2
%
The latter reaction is significant since this oxetane is generally difficult to obtain because large amounts of styrene form readily. 3-Halogenoalkoxides can also be prepared from organotin oxides by a transesterification procedure anal ogous to that published by Matsuda et al. (79); their decomposition normally gives the corresponding oxetane (80). An identical decomposition occurs with 4 - and 5-haloalkoxides leading to tetrahydrofuranes or tetrahydropyranes (81 ), demonstrated by the following examples:
80 ° C
Bu^n—0(CH ) Br 2
4
30min
•
Ο
+
V
Bu SnBr 3
93% 150 °C
Bu£n—0— Br
/
\
Ο \
/
\\
)
/
+
B
U 3
SnBr
Other reactions based on this idea were studied with polyhaloalkoxides which lead to α-halogencarbonyl compounds via a halogenoxirane (isolated in the case of the chloride) (82): Me
I
Me— CH—CHBr J
OSnBu,
no °c 2
30min
Me •
Me C(Br)—CHO
.C—CHBr Me
V
Me 74%
Other heterocycles may also be formed by either geminal or vicinal d i bromides reacting with organotin dialkoxides (83). This route is less easy than the preceding ones although it provides a sometimes useful access to certain dioxanes or dioxolanes:
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
6.
POMMIER
A N D
Bu £nOCH,CH,OSnBu ;
[B
U 3
Alkoxides and Amines
PEREYRE
SnOCH(Me)V
3
+
+
BrCH,CH,Br
°> 48hr
1 7 0
BrCH CH Br 2
\
Ο
2
\) /
Ο
C
72 ihtr
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89
+
Ο
M
+
2Bu SnBr 3
2Bu SnBr e
v
Me
Me
Me ,0-
190 °C
[Bu:3n—0—C(Me) 4r 2
+
Br CH 2
• CH
2
5 days
-Me
/ 2
\
o-
-Me
Me 40%
These reactions are believed to proceed by a two-step mechanism via a halogenalkoxide intermediate. Organotin Alkoxyoxiranes. We have found (84) another interesting and clean intramolecular nucleophilic substitution involving the decomposition or organotin β-alkoxyoxiranes. This reaction led to two different heterocycles depending on the site of attack by the oxygen:
The new organotin alkoxide formed can be readily transformed into the corresponding alcohol by treating it with phthallic acid which precipitates the insoluble organotin phthallate. The orientation of the reaction is mainly a function of the substitution of the oxirane; if the terminal carbon atom of the oxirane is less substituted than the internal one, the formation of the oxetane is largely favored, but if it is equally or more substituted, a tetrahydrofurane is formed. These facts support a mechanism in which a positive charge is developed on the carbons of the oxirane ring in the transition state. A representative se lection of results is given at the top of p. 90.
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
90
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND
APPLICATIONS
Me ( Me ) , C — C H — C H — C H 2
-Me
200 °C, 3hr
84%
2) C H (COOH) 6
4
2
H0CH
OSnBu,
2
Me Me
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A
/λ/γ η/Λ/r χ nC \ τ τ (Me).,C—C(Me),—CH—CH "I " OSnBu,
D 180 C, 3hr 2
M
-Me
e
75%
• 2)C H (COOH), 6
4
HOCH
2
Me
/-\ CH-(LCH 2
OSnBu,
C,H 8
3
°° > C
C H CHO 6
+
5
Br CH 2
+
2
Bu SnBr 3
61%
(^y~OSnBu
+
3
BrCCl
Ç^)^
0
3
+
ŒCl3
+
Bu3SnBr
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70%
C H,MeCHOSnBu G
3
+
BrCCl
3
u-i2LX
C H COMe 6
|>—CHMeOSnBu
3
-I-
BrCCl
m
3
'
\ 14 hr m
5
+
CHC1
+
3
Bu SnBr 3
83%
1 4 h r
Γ>—COMe
+
CHC1
3
+
Bu SnBr 3
50%
The mechanism of this reaction appeared initially to involve abstraction of the hydrogen on the functional carbon atom as a first step followed by the elimination of an organotin free radical:
^ C H — O S n =
+
Q- —
^ C — O S n =
+
QH
l ^ C = 0
+
=Sn-
However, results obtained with the cyclopropyl derivatives (for example to give a cyclic ketone) apparently contradicted this hypothesis. Indeed, our results from the free radical reaction of tin hydrides with cyclopropyl ketones (91) show that the open chain ketones obtained are formed through an intermediate stannyloxy radical: sSnH
Ο
OSn=
QSn
OSn=
The postulated intermediates were the same in the two processes
(>- \— ) è
0Sn
and, to gain insight into this point, we investigated the oxidation of the cyclopropyl derivatives with di-tert-butyl peroxide. The results (90) show that the ketone obtained is mainly the cyclic one but is generally accompanied by a small amount of the open chain compound:
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
6.
M
e
_ ç
— < |
H
OSnBu
M
e
_
c
n
^
M e - C - < ]
3
I
'
Me
cis
PrOOMe
71%
140 c
OSnBu trans
+
95
0
3
29%
ΞΕί2>> M e — C - ^ C l
_ < 1
I
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Alkoxides and Amines
POMMIER AND PEREYRE
\
+ î-BuCOMe +
BuCOMe
3%
10%
1%
8%
Ο Me 8 7 % trans 9 1 % { ^ f 1 6 6 % trans
These observations indicate that the cyclic ketone is the main oxidation product, and, in the case of the ens-2-methylcyclopropyl derivative, an isomerization occurs during the reaction while the open chain ketone is mainly the linear one. The following scheme agrees with all the observations:
±
O-C-R L
Λ
-
Γ>—C—R
Y y 0 8 1 1
+
ssSn-
Ο
In the oxidation case, Reaction c should be favored since no good hydrogen donors are present in the reaction mixture (the only C - H able to act as a donor seems to be the starting alkoxide itself). O n the other hand the relative propor tions of the open chain ketones reflect the thermodynamic stabiility of the two free radicals at equilibrium. The situation is completely different in the tin hydride reduction since the trapping of the radicals once formed is very rapid. The difference between the two types of behavior is very clear if one considers the relative proportions of the open chain ketone obtained: SnH route p>—CH—CH; Me
0 10%
OSnBua
ox. route *
CIS
SnH route
89%
11% (relative)
25%
75%
77%
, . 2 3 % (relative)
CH—CH, Me
OSnBu
3
ύ
trans
v. οχ. route • N
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
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96
ORGANOTIN
COMPOUNDS: N E W
CHEMISTRY A N D
APPLICATIONS
In the tin hydride case, it was found that polar (irans-cyclopropylketone) and stereoelectronic effects (ds-cyclopropylketone) direct the ring opening (92). A n ESR study was then designed in collaboration with A. G. Davies (University College, London) to detect the first formed radical at low temperature. The results (93) show that at —60 °C the photolysis of the organotin cyclopropylmethyl alkoxide in the presence of (ter*-BuO)2, leads to a ring opening, the cis compound giving principally the secondary alkyl radical, and the trans only the primary one. These ESR results concur with the idea of the fast trapping of the initially formed radical by the tin hydride and with an equilibration of the open chain radicals in the absence of a good hydrogen donor via an unstable cyclopropylstannyloxy radical, which in this case, decomposes into the cyclic ketone and a tributylstannyl radical. Two excellent reports have appeared recently in which the organotin alkoxides are very useful intermediates. The first concerns the oxidation of cyclic organotin dialkoxides with bromine which provides a very convenient route to the acyloins (94):
X
C H — C L
X
>nBu
I
2
+
Br
C = 0
| ^CHOH
2
^ C H — C T
+
B SnBr U 2
2
The second procedure involves the oxidation by bromine of various triethyltin alkoxides in the presence of triethyltin methoxide (95). For example: Et SnOMe 3
C H,CH OSnEt; 6
2
3
C H CH,OSnEt 7
1 5
3
+
Br
+
Br,
• QH.CHO
2
E t i S n 0 M
\
C H CHO 7
1 5
+
2Et SnBr
+
MeOH
+
2Et3SnBr
+
MeOH
3
85%
The latter method, however, requires one mole of triethyltin methoxide just to trap the hydrogen bromide. It is probable that this aspect of the reaction can be improved, and that this process will then become a very popular oxidation procedure. Organotin Amines
Like the organotin alkoxides, organotin amines exhibit some quite interesting properties. However, where it is possible to propose several easy preparations of the alkoxides, this is not so for compounds having a tin-nitrogen covalent bond, especially in the case of amino groups R2N where R = alkyl. The only universal method consists of a transmetallation between a lithium or magnesium amine and an organotin halide or oxide, and except in special cases, this method is the
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
6.
POMMIER
A N D
Alkoxides and Amines
PEREYRE
97
most commonly used (see for example 97, 98, 99, 100, 101, 102, 103, 104, 105): lySTM
+
R' SnX
—•
3
R SnKR /
3
2
+
MX
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(M = Li, MgX)
Several other specific routes to the tin amines have been reported although none is generally applicable. Among them, we would like to emphasize the metatheses of organosilicon amines and organotin alkoxides (106), the direct amination of tin halides by amines (107,108,109), and an interfacial technique described by Carraher (110, 111, 112). The first example of a primary organotin amine formed from sterically crowded organotin compounds is also worthy of note (113, 114). For example: KNH
i-Bu SnC,Hô
^
3
*-Bu SnNH 3
2
In spite of the efforts made by several groups of workers (taking account of the number of private communications of unsuccessful attempts) no significant improvement has been found during the past five years. Thus the usefulness of these compounds in synthesis is limited by their difficulty of preparation. However, some properties of the organotin amines are sufficiently interesting to be further studied, and others should be kept in mind until simple preparations make these compounds more readily available. Our group has been involved mainly in substitution and addition reactions, and we report here some of our major results. Nucleophilic Displacement. The reaction of organotin amines with organic halides has been investigated several times and reported as giving either an elimination (115) or, in the more general case, a substitution (116,117,118, 119,120,121,122). During the past five years we have applied this reaction in two special cases: (1) reactions with α-haloketones and (2) reactions of stannazanes with organic dihalides. Reactions of Organotin Amines with a-Haloketones. The overall reaction consists of a substitution of the halogen to form an α-amino ketone (123). For example ^ ^ = 0
+
—• {Z^0
Bu SnNEt2 3
CI
+ Bu3SnC1
NEt, 78%
Me—CO—CH C1 2
+
Bu SnNEt 3
2
—•
Me — C O — C H — N E t 2
2
+
Bu SnCl 3
53% Me—CO—CHC1—Me
+
B
U 3
SnNEt
2
—
Me—CO—CH—Me NEt
+
2
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
Bu SnCl 3
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98
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND APPLICATIONS
Two special features have to be mentioned: (1) contrary to the case of substitution with alkyl halides, all these reactions are exothermic: the experi mental procedure consists only of mixing the two components and distilling immediately the product amino derivative, and (2) the initial step of the reaction is an addition to the carbonyl group as shown by the disappearance of the C = 0 vibration in the IR. From this a mechanism in which the adduct decomposes into an unstable oxirane giving the observed amino ketone by rearrangement can be drawn (124, 125,126): I
OSnBua
I
— C — C —
+ Bu SnNEt 3
2
—
— C — C —
I I X
^ —
X
II X
0
^NEt2 C
' V
x
+
BugSnX
ο
v
NEt2
Î — C — Ο
Ι
NEt
2
However, the observation of the adduct does not indicate that it lies on the reaction coordinate since it is conceivable that it may be the kinetic product of the reaction: .
OSnBu
I I I
— C — C —
II
X
NEt
3
^
— C — C —
+
B
U 3
SnNEt
2
—
I I
Χ
2
I
— C — C —
+
B
U 3
SnX
I I
Ο
Et N
Ο
2
In fact, the pathway by direct substitution must be taken into account in the case of l-chloro-3-pentanone which gives l-diethylamino-3-pentanone in high yield; the formation of an intermediate oxetane is unlikely: Cl—CH —CH —C—Et 2
2
I
+
B
U 3
SnNEt
2
—•
Ο
Et N—CH — CH —C—Et 2
2
2
I ο
+
Bu SnCl 3
It is difficult to choose between these two mechanisms since they would both give the same product (if we admit that during the rearrangement the only migrating group is the amino). For example, 2-chloro-3-pentanone gives 2-diethylamino-3-pentanone as the only product. However, these reactions seem to be very convenient for preparing amino ketones since the above yields correspond to reaction from a stoichiometric
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
6.
99
Alkoxides and Amines
POMMIER AND PEREYRE
mixture of the reactants, and this can be improved by using a slight excess (0.3 M ) of organotin amine: f / = 0
+
Bu SnNEt 3
2
—• Γ Λ = 0
^ < CI
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+
Bu SnCl
1/1:52% L3/l:76%
3
^ < NEt
2
Reactions of Stannazanes with Alkyl Dihalides. We found that the two tin-nitrogen bonds of the stannazanes can be substituted separately:
(Bu Sn) NEt 3
+
2
C H C H C 1 — • BuaSn — 6
5
+
2
Bu SnCl 3
CH C H 2
6
5
70%
Thus, with organic dihalides, it is possible to imagine first a substitution leading to an haloalkylaminotin compound which by cyclization, as in the case of orga notin haloalkoxides, would give a nitrogen heterocycle: Bu Sn—Ν—SnBu 3
+
3
X — X —>
Bu SnN—X — 3
I
I
Et
Et
Bu SnX 3
+ E t —
This reaction proceeds as expected except in the case of the 1,2-dibromoethane where elimination was largely favored. Some problems arose in the case of the 1,3-dibromopropane; it proved impossible to extract the corresponding azetidine from the reaction mixture because of its strong complexation with the organotin bromide. In all the other cases (127), the expected heterocycle was obtained by a continuous distillation of a stoichiometric mixture of dihalide and stannazane. Some characteristic examples are shown below:
(Bu Sn) NEt 3
2
+
BrCH —CH —CHBr—CH 2
2
(Bu Sn) NEt + C I — C H , — C H — C H C 1 — C H 3
2
2
3
—• P i
3
—>• [ j *
K
60% Me
(Bu,Sn) NEt
+
Br(CH ) Br — »
(Bu Sn) NEt
+
Br(CH ,) Br —
2
: i
2
2
L
4
5
[ ^ N — E t
(
Ν—Et
*
65%
60%
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND APPLICATIONS
100
Reactions with Carbonyl Derivatives. O R G A N O T I N A M I N E S A N D A L Organotin amines are now well known to react readily with carbonyl derivatives to give 1,2 dipolar addition (128,129, ISO, 131); this property has been well studied in the case of isocyanates (132,133,134,135,136, 137,138,139,140). For our part, we have investigated the behavior of organotin amines with various carbonyl derivatives and found that the reactions are not generally simple. A n initial paper reports the reaction between organotin amines and acetone as an aldolization owing to the basic properties to the nitrogen atom ( 141 ). However, contrary to this, our preliminary experiments have shown that the reactions with cyclohexanone and cyclopentanone led to the formation of enamines, and with methyl tert-butyl ketone to an organotin enolate (142).
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D E H Y D E S OR K E T O N E S .
(^y==° +
Bu SnNEt 3
*
Ç^y~
NEt
—
2
+
l/2Bu Sn,0 6
+
l/2H 0 2
60% [^)=0
+
Bu SnNEt,
—*
3
Q > — N E t
+
2
l/2B
U 2
Sn 0 2
+
l/2H 0 2
50% Me—CO—ί-Bu
+
Bu SnNEt 3
2
—•
B u S n C H — C O — t-Bu 3
2
66% 60%
/**
+
Et NH 2
BusSn— O — C *-Bu 33%
Lorberth (116) and Manoussakis (143) reported similar findings. To obtain a greater insight into these reactions, we reinvestigated the reaction with acetone itself and found a variety of very different results according to the nature of the amino group involved (144). ο ο ΧΤΛ* Bu SnNMe 3
MeCOMe •
2
C H = C — Me 2
3
+
Me C=CH—C—Me
I
2
"
NMe
32% M r C Q M
%
CH,=C—Me NEt
Bu SnNBu 3
I
0
2
18%
: i
Me,C=CH—C=CH
I
NMe
Bu SnNEt
+
2
2
M e
°°
M e
46%
; !
+ Bu SnCH COMe ;)
2
2
62% > CH =C—Me
8%
2
NBu
2
94%
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
2
2
6.
POMMIER
A N D
Alkoxides and Amines
PEREYRE
101
Mf-OOMp
BuSnNCCftJ,
•
Bu SnCH COMe 3
2
10%
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These different results were rationalized by complementary experiments (145) which led us to conclude that beside the aldolization (observed only when a d i methylamino group is used), two other mechanisms are available: (1) When both the organotin amine and the carbonyl group are not very crowded, an addition followed by elimination occurs leading to an enamine: \
\
^C=0
+
= S n — N =
/
0
S
n
=
—•
—
) —
N
=
+
[=SnOH]
N =
(2) In the other cases, the abstraction of an α-hydrogen occurs to give an organotin enolate: ^C=0
+
—
=Sn—N=
^C=0
H
^
^C—OSn==
+ = N H
S n =
The cases of cyclohexanone and 2-methylcyclohexanone illustrate this point of view; the former gives an enamine, and the latter gives a tin enolate: +
ζ ^ = °
BuaSnNEt*
—
N
E
t
2
+
Bu SnOH 3
60% —CH—CH=CHNEt ( 5
2
+
l/2Bu Sn 0 6
2
+
3
2
1/2C H CH=CH—CHO 6
5
I NEt
2
I
With an excess of tributyltin amine, the enediamine is obtained in 7 5 % yield.
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
104
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND APPLICATIONS
α-Methyl Cinnamaldehyde:
Formation of Enediamine
and Aminal.
II. C
( i
H,—CH=C—CHO
+
2Bu SnNEt 3
2
—*
Me
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Me
I C H —CH=C—CH(NEt ) 6
5
2
+
2
C H 6
—CH—C=CHNEt
5
Me
NEt
II 8 5 %
2
2
15%
f
45 9Ό
β-Methyl Cinnamaldehyde: C H —C=CH—CHO
+
( i
Formation of Dieneamine.
2Bu SnNEt 3
—•
2
III.
C H—C—CH=CH—NEt 6
Me
CH
2
2
70% III
Benzalacetone:
Formation of Organotin Dienolate.
C H5—CH=CH—C—CH 6
+
3
Bu SnNEt 3
2
IV.
—*
0 C H — C H = C H — C—CH^nBu^ +
C H —CH=CH—C=CH
6
6
5
I
2
I
0
Bu SnO 60% 3
40% 60% IV
Benzalacetophenone: Formation of a Reversible 1,4 Adduct. V. This reaction was exothermic and a 1,4 adduct was formed which was identified by N M R . Any attempt at distillation decomposed the product into the starting materials, which distilled together and reacted again in the receiving flask. 0SnBu C„H — C H = C H — C O — C H r>
6
5
+
Bu SnNEt 3
2
^
3
C H — C H — CH=C—C H 6
6
NEt
2
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
5
6.
POMMIER
A N D
Dypnone:
Alkoxides and Amines
PEREYRE
105
Formation of Organotin Dienolate by Elimination.
VI.
Me
I QH-—C=CH—C—C H,
+
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6
Bu SnNEt 3
—•
2
C H — C—CH=C—C H ( i
5
6
I
I
Ο
CH
5
I OSnBu
2
3
78% VI
Except in the case of abstraction of a hydrogen IV, most of the results can be ra tionalized in terms of a 1,4 adduct which is formed either by elimination of amine (III, VI) or via the 3,4 metallotropic form. Indeed, this last compound can either give a β elimination V or add a new molecule of the organotin amine which is followed by elimination I. For this last reaction, we proposed the following mechanism: SnBu
3
eSnNEt«
I
— C — C H = C — O S n =
^
— C—CH—CHO NEt
NEt,
Sn=OSn
I
2
=
I
— C — C H — C H
I
+
I
—•
— C — C H = C H — NEt > +
Bu Sn 0 e
2
I
Et, Ν
NEt
Et N
2
2
To verify this last hypothesis, we investigated the reactions of various organotin enolates to see whether the carbonyl group of the C isomer was able to give normal addition reactions. O R G A N O T I N AMINES A N D O R G A N O T I N E N O L A T E S . We have already seen that organotin enolates exist in two metallotropic forms in equilibrium, the C form having a carbonyl group which may be capable of reacting with organotin amines. Reaction is effectively restricted to those cases where no severe steric hindrance occurs in the C form of the enolates (derivatives of aldehydes and some ketones) (151 ). This fact is indicative of the formation of a transient 1,2 adduct which on decomposition gives an enamine:
^c=r
.
—c-c— 0
S
n
!
S
=Sn
„
e S n N E t 2
105'C,2hr
0 — C — C — N E t , =Sn
I
I
OSns=
— "
"C=C; κ
+ NEt,
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
=Sn,0
106
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND APPLICATIONS
Table I. Starting Carbonyl Derivative
Some E n a m i n e Preparations Yield, %
CSn/OSn, %
Enamine
5/95 5/95
EtCH=CHNEt B u C H = C H — N E t
5/95
Me C=CHNEt
PrCHO C ^ C H O Me. ^ C H — C H O
94% 65%
2
2
2
16%
2
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Me C H
95/5
MeCOMe
2
= C — C H
53%
3
I NEt
30/70
EtCOEt
0%
2
The enamine is formed even in the cases where no detectable C form is present at equilibrium (by N M R ) . Some results are given in Table I. These results also lend support to the mechanism we proposed in the reactions of organotin amines with a-enones. R E A C T I O N S O F S T A N N A Z A N E S W I T H O R G A N O T I N E N O L A T E S . When the organotin amine is replaced by a stannazane in the preceding experiment, we obtained the first example of an organotin eneamine instead of an organic ena mine. OSn—
06n3
5Sn—N—Sn
I I •I I I ===Sn
—*
— C = C — N — Snss
—C—C—Ν—Sns
+
(or
M l
— C — C = N -
sSnOSnï
I =Sn
Under our conditions (150°C, 2 hr), the reaction occurs with the same restrictions as the preceeding one regarding the steric hindrance of the organotin enolate (150). However, by this method, we were able to prepare the organotin eneamines derived from aldehydes and some ketones. Some typical examples are given below: Et
I
Et—CH=CH—Ν—SnBu Et—CH=CH—OSnBu
3
+
(Bu Sn) NEt 3
78%
2
Et—CH—CH=NEt Bi^Sn 22%
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
3
> 49%
6.
POMMIER
A N D
Alkoxides and Amines
PEREYRE
107
Et
I
Bu— Bu—CH=CH—OSnBu
+
3
CH=CH—N—SnBu
3
58%
(Bu Sn) NEt 3
2
Bu — C H — C H = N — E t
I
Bu Sn
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3
14%
CH —C —CH 3
Et Me—CO—CH SnBu 2
3
+
SnBu
(Bu Sn) NEt 3
2
3
40%
79%
2
CH—C—CH^nBu, N—Et 21%
Since this preparative route was rather limited, we investigated several other possible routes. We found particularly that the métallo derivatives of imines react with tributyltin chloride to give the expected derivatiyes; for example, the reaction of tributyltin chloride with a lithium derivative of imine prepared either from a lithium alkyl (150) or, more interestingly from a lithium amide (152). 3 Bu—CH—CH=N—i-Bu
I
Bu Sn 3
BuCH CH=N—i-Bu 2
1) Buli
2)
3 » Bu— CH=CH—N—i-Bu
BU3S11CI
I
Bu Sn 3
Me—CH—CH=N—i-Bu
I
Bu Sn 3
Me—CH —CH=N—;-Bu 2
}
>
2) Bu^nCl
} 70% Me—CH=CH—Ν—i-Bu
I Bu Sn 3
40%
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
108
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND APPLICATIONS Et—CH—CH=N—i-Bu
I
Bu Sn 3
E t — C H o — C H = N — i-Bu
53%
1) i-Pr NIi 2
78%
Et—CH=CH—Ν—i-Bu
2) B u S n C i 3
Bu Sn 3
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47%
These are the reactions of tributyltin chloride with the magnesium deriva tives of imines under more special experimental conditions: Me
SnBih ^ C = C H —
i-Bu
Me 72%
1) t-PrMgCl
/-PrCH=N—i-Bu
2) BugSnCl
Me, C—CH=N—i-Bu Me
SnBu
3
28%
Me
SnBu-3 ^ C = C H — Ν
Me *-PrCH=N-Et
χ
Et
1 ) i P r M g C 1
2) B 3 n C l U 3
M
e
v
C— C H = N — E t
I
Me
SnBu 20% 3
Et
SnBuo
v
^ C = C H — Et E
t
2
_
C
H
=
N
_ ,
B
u
i-Bu
iilf^V 2) BuaSnCl
m
>
5 4 %
^t
C—CH=N—i-Bu Et
SnBu
3
15%
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
6.
POMMIER A N D P E R E Y R E
Alkoxides and Amines
109
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Although these two latter pathways are known to work more readily with hindered imines while the reverse is true for the method via the organotin enolates, we think we have developed a sufficient set of preparative routes to obtain most organotin eneamines. At this time, studies of the metallotropic equilibrium between the C and Ν organotin isomers and also of the reactivity of these com pounds are in progress. Acknowledgments The authors thank J. Valade who initiated organotin chemistry in Bordeaux for his stimulating interest; to J. A. Richards for checking the manuscript and to M . F. Penna for accurate and patient typing.
Literature Cited 1. 2. 3. 4. 5. 6. 7. 8. 9. 10. 11. 12. 13. 14. 15. 16. 17. 18. 19. 20. 21. 22. 23. 24. 25. 26. 27. 28. 29. 30.
Neumann, W. P., "The Organic Chemistry of Tin," Wiley, New York, 1970. Poller, R. C., "The Chemistry of Organotin Compounds,' Logos, London, 1970. Sawyer, A. K., "Organotin Compounds," Vols. I, II, III, Dekker, New York, 1971. Smith, J. D., Walton, D. R. M., in "Advances in Organometallic Chemistry," Vol. 13, F. G. A. Stone and R. West Eds., p. 453 Academic, New York, 1975. Bloodworth, A. J., Davies, A. G., Chem. Ind., London (1972) 12, 490. Davies, A. G., Synthesis (1969) 56. Jones, K., Lappert, M. F., Organomet. Chem. Rev. (1966) 1, 67. Davies, A. G., Palan, P. R., Vasishta, S. C., Chem. Ind. (1967) 229. Davies, A. G., U.S. Patent, 3, 492,327; Chem. Abs. (1970) 72, 90638. Davies, A. G., Kleinschmidt, D. C., Palan, P. R., Vasishta, S. C., J. Chem. Soc., C, (1971) 3972. Sakai, S., Fujimura, Y., Ishii, Y., Org. Chem. (1970) 2344. David, S., Thieffry, Α., C. R. Acad.Sci.,Ser., C (1974) 279, 1045. Gaur, D. P., Srivastava, G., Mehrotra, R. C., J. Organometal. Chem. (1974) 65, 195. Jones, K., Lappert, M. F., Proc. Chem. Soc. (1964) 22. Mehrotra, R. C., Bachlas, B. P., J. Organometal. Chem. (1970) 22, 121. Dubukina, Ο. V., Lutsenko, I. F , Zh. Obsch. Chim. (1970) 40, 2766. Gaur, D. P., Srivastava, G., Mehrotra, R. C., J. Organometal. Chem. (1973) 63, 213. Azerbaev, I. N., Erzhanov, Κ. B., Polatebekov, N. P., Kochin, D. Α., Izv. Akad. Νauk. Kaj. SSR, Ser. Khim. (1972) 22, 50. Voronkov, M. G., Ivanova, N. P., Timilova, L. F, Mirskov, R. G., Dolk. Vsas, Kouf. Khim. Atsatilana, 4th (1972) 2, 188; Chem. Abs. (1973) 79, 78898. George, Τ. Α., Jones, K., Lappert, M. F., J. Chem. Soc. (1965) 2157. Mehrotra, R. C., Bachlas, B. P., J. Organometal. Chem. (1970) 22, 129. Tzschach, Α., Ponicke, Κ., Z. Anorg. Allg. Chem. (1974) 404, 121. Wagner, D., Verheyden, J. P. H., Moffat, J. G., J. Org. Chem. (1974) 39, 24. Baur, D. P., Srivastava, G., Mehrotra, R. C., J. Organometal. Chem. (1973) 63, 221. Harrison, P. G., Zuckerman, J. J., Inorg. Nucl. Chem. Lett. (1970) 6, 5. Allan, M., Ianzen, A. F., Willis, C., Can. J. Chem. (1968) 46, 3671. Gaur, D. P., Srivastava, G., Mehrotra, R. C., J. Organometal. Chem. (1973) 47, 95. Harrison, P. G., Zuckerman, J. J., Inorg. Chem. Acta. (1970) 4, 235. Kennedy, J. D., J. Chem.Soc.,Perkin II (1973) 1785. Lorbert, J., Kula, M. R., Chem. Ber. (1964) 97, 3444.
In Organotin Compounds: New Chemistry and Applications; Zuckerman, J.; Advances in Chemistry; American Chemical Society: Washington, DC, 1976.
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110
ORGANOTIN COMPOUNDS: NEW CHEMISTRY AND APPLICATIONS
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